Literature DB >> 33527780

Mesenchymal stromal cell delivery via an ex vivo bioreactor preclinical test system attenuates clot formation for intravascular application.

Brian O'Rourke1, Sunny Nguyen1, Arno W Tilles1, James A Bynum2, Andrew P Cap2, Biju Parekkadan1,3,4,5, Rita N Barcia1.   

Abstract

While mesenchymal stromal cells are an appealing therapeutic option for a range of clinical applications, their potential to induce clotting when used systemically remains a safety concern, particularly in hypercoagulable conditions, such as in patients with severe COVID-19, trauma, or cancers. Here, we tested a novel preclinical approach aimed at improving the safety of mesenchymal stromal cell (MSC) systemic administration by use of a bioreactor. In this system, MSCs are seeded on the exterior of a hollow-fiber filter, sequestering them behind a hemocompatible semipermeable membrane with defined pore-size and permeability to allow for a molecularly defined cross talk between the therapeutic cells and the whole blood environment, including blood cells and signaling molecules. The potential for these bioreactor MSCs to induce clots in coagulable plasma was compared against directly injected "free" MSCs, a model of systemic administration. Our results showed that restricting MSCs exposure to plasma via a bioreactor extends the time necessary for clot formation to occur when compared with "free" MSCs. Measurement of cell surface data indicates the presence of known clot inducing factors, namely tissue factor and phosphatidylserine. Results also showed that recovering cells and flushing the bioreactor prior to use further prolonged clot formation time. Furthermore, application of this technology in two in vivo models did not require additional heparin in fully anticoagulated experimental animals to maintain target activated clotting time levels relative to heparin anticoagulated controls. Taken together the clinical use of bioreactor housed MSCs could offer a novel method to control systemic MSC exposure and prolong clot formation time.
© 2021 The Authors. STEM CELLS TRANSLATIONAL MEDICINE published by Wiley Periodicals LLC on behalf of AlphaMed Press.

Entities:  

Keywords:  COVID-19; IBMR; bioreactor; clot formation time; clotting; ex vivo; heparin; hypercoagulable; instant blood-mediated inflammatory reaction; mesenchymal stromal cells; perfusion

Year:  2021        PMID: 33527780     DOI: 10.1002/sctm.20-0454

Source DB:  PubMed          Journal:  Stem Cells Transl Med        ISSN: 2157-6564            Impact factor:   6.940


  4 in total

1.  Improved MSC Minimal Criteria to Maximize Patient Safety: A Call to Embrace Tissue Factor and Hemocompatibility Assessment of MSC Products.

Authors:  Guido Moll; James A Ankrum; Scott D Olson; Jan A Nolta
Journal:  Stem Cells Transl Med       Date:  2022-03-03       Impact factor: 7.655

2.  Advanced cell therapy with low tissue factor loaded product NestaCell® does not confer thrombogenic risk for critically ill COVID-19 heparin-treated patients.

Authors:  Rodrigo Pinheiro Araldi; Benedito Carlos Prezoto; Vivian Gonzaga; Bruna Policiquio; Thais Biude Mendes; Fernanda D'Amélio; Hugo Vigerelli; Mariana Viana; Cristiane Wenceslau Valverde; Eduardo Pagani; Irina Kerkis
Journal:  Biomed Pharmacother       Date:  2022-04-01       Impact factor: 7.419

Review 3.  Mesenchymal stem cells and their derived small extracellular vesicles for COVID-19 treatment.

Authors:  Yuling Huang; Xin Li; Lina Yang
Journal:  Stem Cell Res Ther       Date:  2022-08-12       Impact factor: 8.079

4.  Pharmacological effects of ex vivo mesenchymal stem cell immunotherapy in patients with acute kidney injury and underlying systemic inflammation.

Authors:  Madhav Swaminathan; Nelson Kopyt; Mohamed G Atta; Jai Radhakrishnan; Kausik Umanath; Sunny Nguyen; Brian O'Rourke; Ashley Allen; Natalie Vaninov; Arno Tilles; Elizabeth LaPointe; Andrew Blair; Chris Gemmiti; Brian Miller; Biju Parekkadan; Rita N Barcia
Journal:  Stem Cells Transl Med       Date:  2021-09-28       Impact factor: 6.940

  4 in total

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